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血液与贵金属的相互作用:凝血和免疫补体激活。

Blood interactions with noble metals: coagulation and immune complement activation.

机构信息

Department of Cell and Molecular Biology/Interface Biophysics, Gothenburg University, Medicinaregatan 9E, 41390 Gothenburg, Sweden.

出版信息

ACS Appl Mater Interfaces. 2009 May;1(5):1053-62. doi: 10.1021/am900028e.

Abstract

Noble metals are interesting biomaterials for a number of reasons, e.g., their chemical inertness and relative mechanical softness, silver's long known antimicrobial properties, and the low allergenic response shown by gold. Although important for the final outcome of biomaterials, little is reported about early events between pure noble metals and blood. In this article, we used whole blood in the "slide chamber model" to study the activation of the immune complement activation, generation of thrombin/antithrombin (TAT) complexes, and platelet depletion from blood upon contact with silver (Ag), palladium (Pd), gold (Au), titanium (Ti), and Bactiguard, a commercial nanostructured biomaterial coating comprised of Ag, Pd, and Au. The results show the highest TAT generation and platelet depletion on Ti and Au and lower on Pd, Ag, and the Bactiguard coating. The immune complement factor 3 fragment (C3a) was generated by the surfaces in the following order: Ag > Au > Pd > Bactiguard > Ti. Quartz crystal microbalance adsorption studies with human fibrinogen displayed the highest deposition to Ag and the lowest onto the Bactiguard coating. The adsorbed amounts of fibrinogen did not correlate with thrombogenicity in terms of TAT formation and platelet surface accumulation in blood. The combined results suggest, hence, that noble metal chemistry has a different impact on the protein adsorption properties and general blood compatibility. The low thrombogenic response by the Bactiguard coating cannot be explained by any of the single noble metal properties but is likely a successful combination of the nanostructure, nanogalvanic effects, or combinatory chemical and physical materials properties.

摘要

贵金属因其诸多特性而成为有趣的生物材料,例如它们的化学惰性和相对柔软的机械特性、银的长期抗菌性能以及金的低致敏反应。尽管这些特性对于生物材料的最终结果非常重要,但关于纯贵金属与血液之间的早期相互作用,人们知之甚少。在本文中,我们使用全血在“滑动室模型”中研究了免疫补体激活、凝血酶/抗凝血酶(TAT)复合物的生成以及与银(Ag)、钯(Pd)、金(Au)、钛(Ti)和 Bactiguard 接触时血液中血小板的耗竭,Bactiguard 是一种由 Ag、Pd 和 Au 组成的商业纳米结构生物材料涂层。结果表明,Ti 和 Au 上的 TAT 生成和血小板耗竭最高,Pd、Ag 和 Bactiguard 涂层则较低。表面依次生成免疫补体因子 3 片段(C3a):Ag > Au > Pd > Bactiguard > Ti。人纤维蛋白原在石英晶体微天平吸附研究中显示,Ag 的沉积量最高,而 Bactiguard 涂层的沉积量最低。纤维蛋白原的吸附量与 TAT 形成和血小板在血液中的表面积累方面的血栓形成性无关。因此,综合结果表明,贵金属化学对蛋白质吸附特性和整体血液相容性具有不同的影响。Bactiguard 涂层的低血栓形成反应不能用任何单一贵金属性质来解释,而是可能是纳米结构、纳米电偶效应或组合化学和物理材料性质的成功结合。

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